1 pentyl 3 phenylacetylindoles a new class of cannabimimetic indoles bioorg med chem lett 15 4110 4113 (2005)


Bioorganic & Medicinal Chemistry Letters 15 (2005) 4110 4113
1-Pentyl-3-phenylacetylindoles, a new class of
cannabimimetic indoles
John W. Huffman,a,* Paul V. Szklennik,a Amanda Almond,a Kristen Bushell,a
Dana E. Selley,b Hengjun He,b Michael P. Cassidy,b Jenny L. Wileyb and Billy R. Martinb
a
Howard L. Hunter Laboratory, Clemson University, Clemson, SC 29634-0973, USA
b
Department of Pharmacology and Toxicology, Medical College of Virginia Campus, Virginia Commonwealth University,
Richmond, VA 23298-0613, USA
Received 12 May 2005; revised 30 May 2005; accepted 2 June 2005
Available online 6 July 2005
Abstract A new class of cannabimimetic indoles, with 3-phenylacetyl or substituted 3-phenylacetyl substituents, has been prepared
and their affinities for the cannabinoid CB1 and CB2 receptors have been determined. In general those compounds with a 2-substi-
tuted phenylacetyl group have good affinity for both receptors. The 4-substituted analogs have little affinity for either receptor, while
the 3-substituted compounds are intermediate in their affinities. Two of these compounds, 1-pentyl-3-(2-methylphenylacetyl)indole
(JWH-251) and 1-pentyl-3-(3-methoxyphenylacetyl)indole (JWH-302), have 5-fold selectivity for the CB1 receptor with modest affin-
ity for the CB2 receptor. GTPcS determinations indicate that both compounds are highly efficacious agonists at the CB1 receptor
and partial agonists at the CB2 receptor.
Ó 2005 Elsevier Ltd. All rights reserved.
In the classical investigation of the structure activity hydro-1-naphthoyl) compound had moderate affinity
relationships (SAR) of cannabimimetic aminoalkyl- for the CB1 receptor and was quite potent in inhibiting
indoles, such as WIN-55,212-2 (1), it was found that a the electrically induced contractions of the isolated
3-(1-naphthoyl) substituent appended to the indole mouse vas deferens. The compound with a 3-(5,6,7,8-tet-
nucleus provided greater affinity for the cannabinoid rahydro-1-naphthoyl) substituent had considerably less
CB1 receptor than a substituted benzoyl group.1 Nearly affinity for the receptor, but was slightly more potent
simultaneously, we demonstrated that the N-aminoalkyl than the 1,2,3,4-tetrahydro-1-naphthoyl analog in the
group could be replaced by an alkyl group without loss mouse vas deferens protocol. It was suggested that the
of cannabinoid activity. An n-pentyl group on the indole potency of these compounds is due to the presence of
nitrogen, as in JWH-018 (2), provided maximum affinity a bicyclic substituent at C-3 of the indole, rather than
for the CB1 receptor, and in vivo potency typical of tra- to specific aromatic interactions. However, there now
ditional cannabinoids, such as D9-tetrahydrocannabinol exists convincing evidence that cannabimimetic indoles,
(3, D9-THC).2,3 Subsequently, we prepared a number of including aminoalkylindoles, interact with the CB1
N-alkyl 3-(1-naphthoyl)indole derivatives to develop receptor primarily by aromatic stacking.8,9
SAR for cannabimimetic indoles at both the CB1 and
CB2 receptors.4 7 There appeared to be two plausible explanations for
the greatly enhanced CB1 receptor affinities of the 3-
Among the compounds included in the study by (1-naphthoyl)indoles. Either the presence of a second
the Winthrop group were aminoalkylindoles with aromatic ring increased the magnitude of stacking inter-
3-(1,2,3,4-tetrahydro-1-naphthoyl) and 3-(5,6,7,8-tetra- actions with the CB1 receptor or the geometry of the
hydro-1-naphthoyl) substituents.1 The 3-(1,2,3,4-tetra- naphthoyl indoles is such that the second aromatic ring
(carbons 5 8) is proximate to aromatic amino acids in
the receptor, which would increase the stacking interac-
Keywords: Cannabinoids; Structure activity relationships; Cannabi-
tions. To gain evidence regarding this question, we pre-
noid receptors; Aminoalkylindole.
* pared a series of 1-pentyl-3-phenylacetylindoles (4,
Corresponding author. Tel.: +1 86 4656 3133; fax: +1 86 4656
6613; e-mail: huffman@clemson.edu Scheme 1). These indole derivatives include compounds
0960-894X/$ - see front matter Ó 2005 Elsevier Ltd. All rights reserved.
doi:10.1016/j.bmcl.2005.06.008
J. W. Huffman et al. / Bioorg. Med. Chem. Lett. 15 (2005) 4110 4113 4111
both with and without a C-2 methyl substituent (4, JWH-304) have uniformly low CB1 receptor affinity
R=CH3 or H). A variety of compounds were synthe- (Ki = 179 3363 nM).
sized, including those with methyl-, methoxy-, fluoro-,
chloro-, and bromophenyl substituents as well as the The 3-(2-substituted phenylacetyl)indoles have good to
unsubstituted analogs. high affinity for the CB1 receptor. The highest affinity
compounds are 1-pentyl-3-(2-chlorophenylacetyl)indole
Cannabimimetic indoles were synthesized from 1- (JWH-203), with Ki = 8.0 Ä… 0.9 nM and 1-pentyl-3-
pentylindole (5, R = H) or 2-methyl-1-pentylindole (5, (2-bromophenylacetyl)indole (JWH-249) Ki = 8.4 Ä…
R=CH3) and the appropriate phenylacetyl chloride 1.8 nM. 1-Pentyl-2-methyl-3-(2-methoxyphenylace-
by the Okauchi modification of the Friedel Crafts reac- tyl)indole (JWH-306), the 1-pentyl-3-(2-fluoropheny-
tion (Scheme 1).7,10 In this procedure the substrate in- lacetyl)indoles (JWH-311 and JWH-314), and the
dole is stirred in dichloromethane with 1.5 equiv of 1-pentyl-3-(2-methylphenylacetyl)indoles (JWH-251 and
dimethylaluminum chloride at 0 °C for up to 1 h. To this JWH-252) have the lowest affinities of this group of
intermediate organoaluminum compound is added compounds with Ki = 23 39 nM. The other 3-(2-substi-
1.5 equiv of the acyl halide.11 Evidence for the forma- tuted phenylacetyl)indoles, JWH-204, JWH-305, and
tion of an organoaluminum intermediate follows from JWH-250 have Ki = 11 15 nM.
the observation that reaction of 1-pentylindole with
dimethylaluminum chloride and quenching with D2O Those compounds with a 3-substituted phenylacetyl
provided 3-deuterio-1-pentylindole. group have CB1 receptor affinities intermediate between
those of the 2- and 4-substituted analogs. In particular,
The affinities of the phenylacetylindoles for the CB1 recep- 1-pentyl-3-(3-methoxyphenylacetyl)indole (JWH-302,
tor were determined by measuring their ability to displace Ki = 17 Ä… 2 nM) and 1-pentyl-3-(3-chlorophenylace-
[3H]CP-55,940 from its binding site in a membrane prep- tyl)indole (JWH-237, Ki = 38 Ä… 10 nM) have quite high
aration from rat brain,12 and CB2 receptor affinities were affinity for the CB1 receptor. The corresponding 2-
determined by measuring the ability of the compounds to methylindoles (JWH-253 and JWH-303) have significant-
displace [3H]CP-55,940 from a cloned human receptor ly lower affinities than JWH-237 and JWH-302. Both
preparation.13 The results of these determinations are 1-pentyl-3-(3-fluorophenylacetyl)indole (JWH-312) and
summarized in Table 1. The receptor affinities for WIN- the corresponding 2-methylindole (JWH-315) have mod-
55,212-2 (1) and D9-THC (3) are also included in Table 1. est and little affinity, respectively, for the CB1 receptor.
The receptor affinities summarized in Table 1 indicate In general the CB2 receptor affinities of this class of in-
that in general the 2-methylindoles have lower affinity doles follow the same trend as their CB1 affinities (Table
for the CB1 receptor than the 2-unsubstituted analogs. 1). That is, the 2-substituted phenylacetyl compounds
This is a general trend in the cannabimimetic indole ser- have the greatest affinity, followed by the 3-substituted
ies.1,3 5,7 The compounds with an unsubstituted pheny- analogs. The 3-(4-substituted phenylacetyl)indoles have
lacetyl group (JWH-167 and JWH-205) have modest negligible affinity for the CB2 receptor, and most of
affinities (Ki = 90 Ä… 17 nM and 124 Ä… 23 nM, respective- the 2-methylindoles have lower CB2 receptor affinities
ly) for the CB1 receptor. The 4-substituted analogs than the unsubstituted analogs. However, in the 1-pen-
(JWH-208, JWH-209, JWH-201, JWH-202, JWH-313, tyl-3-(2-methylphenylacetyl)indoles the 2-methylindole
JWH-316, JWH-206, JWH-207, JWH-248, and analog (JWH-252, Ki = 19 Ä… 1 nM) has more than
Scheme 1.
4112 J. W. Huffman et al. / Bioorg. Med. Chem. Lett. 15 (2005) 4110 4113
Table 1. Receptor affinities (mean Ä… SEM) of 1-pentyl-3-phenylacetylindoles
3-Substituent R Ki (nM)
CB1 CB2 Ratio CB1/CB2
WIN-55,212-2 (1) 1.9 Ä… 0.1a 0.28 Ä… 0.16a 6.8
D9-THC (3)41 Ä… 2b 36 Ä… 10a 1.1
Phenylacetyl, JWH-167 H 90 Ä… 17 159 Ä… 14 0.57
Phenylacetyl, JWH-205 CH3 124 Ä… 23 180 Ä… 9 0.69
2-Methylphenylacetyl, JWH-251 H 29 Ä… 3 146 Ä… 36 0.20
2-Methylphenylacetyl, JWH-252 CH3 23 Ä… 3 19 Ä… 1 1.2
4-Methylphenylacetyl, JWH-208 H 179 Ä… 7 570 Ä… 127 0.31
4-Methylphenylacetyl, JWH-209 CH3 746 Ä… 49 1353 Ä… 270 0.55
2-Methoxyphenylacetyl, JWH-250 H 11 Ä… 2 33 Ä… 2 0.33
2-Methoxyphenylacetyl, JWH-306 CH3 25 Ä… 1 82 Ä… 11 0.30
3-Methoxyphenylacetyl, JWH-302 H 17 Ä… 2 89 Ä… 15 0.19
3-Methoxyphenylacetyl, JWH-253 CH3 62 Ä… 10 84 Ä… 12 0.74
4-Methoxyphenylacetyl, JWH-201 H 1064 Ä… 21 444 Ä… 14 2.4
4-Methoxyphenylacetyl, JWH-202 CH3 1678 Ä… 63 645 Ä… 6 2.6
2-Fluorophenylacetyl, JWH-311 H 23 Ä… 2 39 Ä… 3 0.60
2-Fluorophenylacetyl, JWH-314 CH3 39 Ä… 2 76 Ä… 4 0.51
3-Fluorophenylacetyl, JWH-312 H 72 Ä… 7 91 Ä… 20 0.79
3-Fluorophenylacetyl, JWH-315 CH3 430 Ä… 24 182 Ä… 23 2.4
4-Fluorophenylacetyl, JWH-313 H 422 Ä… 19 365 Ä… 92 1.2
4-Fluorophenylacetyl, JWH-316 CH3 2862 Ä… 670 781 Ä… 105 3.7
2-Chlorophenylacetyl, JWH-203 H 8.0 Ä… 0.9 7.0 Ä… 1.3 1.1
2-Chlorophenylacetyl, JWH-204 CH3 13 Ä… 1 25 Ä… 1 0.52
3-Chlorophenylacetyl, JWH-237 H 38 Ä… 10 106 Ä… 2 0.36
3-Chlorophenylacetyl, JWH-303 CH3 117 Ä… 10 138 Ä… 12 0.85
4-Chlorophenylacetyl, JWH-206 H 389 Ä… 25 498 Ä… 37 0.78
4-Chlorophenylacetyl, JWH-207 CH3 1598 Ä… 134 3723 Ä… 10 0.43
2-Bromophenylacetyl, JWH-249 H 8.4 Ä… 1.8 20 Ä… 2 0.42
2-Bromophenylacetyl, JWH-305 CH3 15 Ä… 1.8 29 Ä… 5 0.52
4-Bromophenylacetyl, JWH-248 H 1028 Ä… 39 657 Ä… 19 1.6
4-Bromophenylacetyl, JWH-304 CH3 3363 Ä… 332 2679 Ä… 688 1.2
a
Ref. 13.
b
Ref. 12.
7-fold greater affinity for the CB2 receptor than the cannabinoid full agonist. JWH-251 and JWH-302 both
unsubstituted compound (JWH-251, Ki = 146 Ä… 36 nM). stimulate GTPcS binding at CB1, with approximately
equal values of EC50 (29 nM) and are high efficacy ago-
In contrast to most cannabimimetic indoles, which tend nists with Emax of greater than 90% (Table 2). Although
to show selectivity for the CB2 receptor,4,6,7,13 two of the affinities of these compounds at CB2 are approxi-
these phenylacetylindoles show 5-fold selectivity for mately one-fifth that of their affinities for the CB1 recep-
the CB1 receptor. One of them, 1-pentyl-3-(2-methylph- tor, both significantly stimulate GTPcS binding at the
enylacetyl)indole, JWH-251, has good affinity for the CB2 receptor. Surprisingly, their potencies for CB2
CB1 receptor (Ki = 29 Ä… 3 nM) with modest affinity for receptor activation were similar to those seen with
the CB2 receptor (Ki = 146 Ä… 36 nM). The other, 1-pen- CB1: for JWH-251, EC50 = 8.3 Ä… 0.8 nM and for JWH-
tyl-3-(3-methoxyphenylacetyl)indole, JWH-302, also has 302, EC50 = 24.4 Ä… 6.9 nM. At the CB2 receptor, howev-
good affinity (Ki = 17 Ä… 2 nM) for the CB1 receptor, and er, both compounds are partial agonists with Emax val-
fair affinity for the CB2 receptor (Ki = 89 Ä… 15 nM). To ues of less than 50%.
evaluate the efficacy of these compounds, their ability
to stimulate [35S]GTPcS binding at CB1 and CB2 was The 1-pentyl-3-phenylacetylindoles constitute a new
determined.7,14 The results of these determinations class of cannabimimetic indoles, which in contrast to
are summarized in Table 2, where the stimulation most compounds of this general type show little selectiv-
produced at each receptor is normalized to a standard ity for the CB2 receptor. Two of these indole derivatives,
Table 2. EC50 and Emax values (mean Ä… SEM) for stimulation by GTPcS binding of CB1 and CB2 for JWH-251 and JWH-302
Compound CB1a CB2a
EC50 (nM) Emax (%) EC50 (nM) Emax (%)
1-Pentyl-3-(2-methylphenylacetyl)indole (JWH-251) 29.0 Ä… 5.5 97.6 Ä… 1.5 8.3 Ä… 0.8 47.0 Ä… 2.4
1-Pentyl-3-(3-methoxyphenylacetyl)indole (JWH-302) 29.3 Ä… 0.8 91.5 Ä… 2.9 24.4 Ä… 6.9 33.5 Ä… 2.9
a
Stimulation values are from data normalized to stimulation produced by a maximally effective concentration of a standard full agonist: 10 lM
WIN-55,212-2 for CB1 and 3 lM CP-55,940 for CB2 receptors.
J. W. Huffman et al. / Bioorg. Med. Chem. Lett. 15 (2005) 4110 4113 4113
3. Wiley, J. L.; Compton, D. R.; Dai, D.; Lainton, J. A. H.;
JWH-251 and JWH-302, are moderately selective for the
Phillips, M.; Huffman, J. W.; Martin, B. R. J. Pharmacol.
CB1 receptor and are full agonists at this receptor. Selec-
Exp. Ther. 1998, 285, 995.
tive agonists for the CB1 receptor are relatively rare and
4. Aung, M. M.; Griffin, G.; Huffman, J. W.; Wu, M.-J.;
although these compounds are also partial agonists at
Keel, C.; Yang, B.; Showalter, V. M.; Abood, M. E.;
the CB2 receptor, they may serve as the prototypes for
Martin, B. R. Drug Alcohol Depend. 2000, 60, 133.
additional CB1 receptor selective agonists. In addition,
5. Huffman, J. W. Curr. Med. Chem. 1999, 6, 705.
the high CB1 receptor affinities of several of these com-
6. Huffman, J. W. Curr. Pharm. Des. 2000, 6, 1323.
pounds combined with the efficacies of JWH-251 and
7. Huffman, J. W.; Zengin, G.; Wu, M.-J.; Lu, J.; Hynd,
JWH-302 suggest that the increased potency of cannab-
G.; Bushell, K.; Thompson, A.; Bushell, S.; Tartal, C.;
imimetic 3-(1-naphthoyl)indoles relative to their benzoyl Hurst, D. P.; Reggio, P. H.; Selley, D. E.; Cassidy, M.
P.; Wiley, J. L.; Martin, B. R. Bioorg. Med. Chem. 2005,
congeners is caused by their molecular geometry rather
13, 89.
than the presence of a second aromatic ring.
8. Reggio, P. H.; Basu-Dutt, S.; Barnett-Norris, J.; Castro,
M. T.; Hurst, D. P.; Seltzman, H. H.; Roche, M. J.;
Gilliam, A. F.; Thomas, B. F.; Stevenson, L. A.; Pertwee,
Acknowledgments
R. G.; Abood, M. E. J. Med. Chem. 1998, 41, 5177.
9. Huffman, J. W.; Mabon, R.; Wu, M.-J.; Lu, J.; Hart, R.;
The work at Clemson was supported by Grants Hurst, D. P.; Reggio, P. H.; Wiley, J. L.; Martin, B. R.
DA03590 and DA15340 to J.W.H., that at Virginia Bioorg. Med. Chem. 2003, 11, 539.
10. Okauchi, T.; Itonaga, M.; Minami, T.; Owa, T.; Kitoh,
Commonwealth University by Grant DA03672 to
K.; Yoshino, H. Org. Lett. 2000, 2, 1485.
B.R.M. and DA05274 to D.E.S., all from the National
11. The phenylacetyl indoles were formed in unoptimized
Institute on Drug Abuse.
yields of 32 72%. All target compounds have mass
1 13
spectral, H, and C NMR data consistent with the
assigned structures. All compounds gave acceptable
References and notes
microanalytical or high-resolution mass spectral data.
12. Compton, D. R.; Rice, K. C.; De Costa, B. R.; Razdan,
1. Eissenstat, M. A.; Bell, M. R.; DÕAmbra, T. E.; Alexander, R. K.; Melvin, L. S.; Johnson, M. R.; Martin, B. R.
E. J.; Daum, S. J.; Ackerman, J. H.; Gruett, M. D.; Kumar, J. Pharmacol. Exp. Ther. 1993, 265, 218.
V.; Estep, K. G.; Olefirowicz, E. M.; Wetzel, J. R.; 13. Showalter, V. M.; Compton, D. R.; Martin, B. R.; Abood,
Alexander, M. D.; Weaver, J. D.; Haycock, D. A.; Luttin- M. E. J. Pharmacol. Exp. Ther. 1996, 278, 989.
ger, D. A.; Casiano, F. M.; Chippari, S. M.; Kuster, J. E.; 14. Selley, D. E.; Stark, S.; Sim, L. J.; Childers, S. R. Life Sci.
Stevenson, J. I.; Ward, S. J. J. Med. Chem. 1995, 38, 3094. 1996, 59, 659, Chinese hamster ovary (CHO) cells stably
2. Huffman, J. W.; Dai, D.; Martin, B. R.; Compton, D. R. expressing the human CB1 or CB2 receptor were employed
Bioorg. Med. Chem. Lett. 1994, 4, 563. in this determination.


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